Your search keyword '"Mijoon Lee"' showing total 200 results

1. Molecular basis of the final step of cell division in Streptococcus pneumoniae

Author

Siseth Martínez-Caballero, Céline Freton, Rafael Molina, Sergio G. Bartual, Virginie Gueguen-Chaignon, Chryslène Mercy, Federico Gago, Kiran V. Mahasenan, Inés G. Muñoz, Mijoon Lee, Dusan Hesek, Shahriar Mobashery, Juan A. Hermoso, and Christophe Grangeasse

Subjects

CP: Microbiology, Biology (General), QH301-705.5

Abstract

Summary: Bacterial cell-wall hydrolases must be tightly regulated during bacterial cell division to prevent aberrant cell lysis and to allow final separation of viable daughter cells. In a multidisciplinary work, we disclose the molecular dialogue between the cell-wall hydrolase LytB, wall teichoic acids, and the eukaryotic-like protein kinase StkP in Streptococcus pneumoniae. After characterizing the peptidoglycan recognition mode by the catalytic domain of LytB, we further demonstrate that LytB possesses a modular organization allowing the specific binding to wall teichoic acids and to the protein kinase StkP. Structural and cellular studies notably reveal that the temporal and spatial localization of LytB is governed by the interaction between specific modules of LytB and the final PASTA domain of StkP. Our data collectively provide a comprehensive understanding of how LytB performs final separation of daughter cells and highlights the regulatory role of eukaryotic-like kinases on lytic machineries in the last step of cell division in streptococci.

Published

2023

2. Integrative structural biology of the penicillin-binding protein-1 from Staphylococcus aureus, an essential component of the divisome machinery

Author

Siseth Martínez-Caballero, Kiran V. Mahasenan, Choon Kim, Rafael Molina, Rhona Feltzer, Mijoon Lee, Renee Bouley, Dusan Hesek, Jed F. Fisher, Inés G. Muñoz, Mayland Chang, Shahriar Mobashery, and Juan A. Hermoso

Subjects

Divisome, Staphylococcus aureus, X-ray crystal structure, SAXS in-solution structure, Molecular dynamics simulations, PBP1, Biotechnology, TP248.13-248.65

Abstract

The penicillin-binding proteins are the enzyme catalysts of the critical transpeptidation crosslinking polymerization reaction of bacterial peptidoglycan synthesis and the molecular targets of the penicillin antibiotics. Here, we report a combined crystallographic, small-angle X-ray scattering (SAXS) in-solution structure, computational and biophysical analysis of PBP1 of Staphylococcus aureus (saPBP1), providing mechanistic clues about its function and regulation during cell division. The structure reveals the pedestal domain, the transpeptidase domain, and most of the linker connecting to the “penicillin-binding protein and serine/threonine kinase associated” (PASTA) domains, but not its two PASTA domains, despite their presence in the construct. To address this absence, the structure of the PASTA domains was determined at 1.5 Å resolution. Extensive molecular-dynamics simulations interpret the PASTA domains of saPBP1 as conformationally mobile and separated from the transpeptidase domain. This conclusion was confirmed by SAXS experiments on the full-length protein in solution. A series of crystallographic complexes with β-lactam antibiotics (as inhibitors) and penta-Gly (as a substrate mimetic) allowed the molecular characterization of both inhibition by antibiotics and binding for the donor and acceptor peptidoglycan strands. Mass-spectrometry experiments with synthetic peptidoglycan fragments revealed binding by PASTA domains in coordination with the remaining domains. The observed mobility of the PASTA domain in saPBP1 could play a crucial role for in vivo interaction with its glycosyltransferase partner in the membrane or with other components of the divisome machinery, as well as for coordination of transpeptidation and polymerization processes in the bacterial divisome.

Published

2021

3. C6 Hydroxymethyl-Substituted Carbapenem MA-1-206 Inhibits the Major Acinetobacter baumannii Carbapenemase OXA-23 by Impeding Deacylation

Author

Nichole K. Stewart, Marta Toth, Maha A. Alqurafi, Weirui Chai, Thu Q. Nguyen, Pojun Quan, Mijoon Lee, John D. Buynak, Clyde A. Smith, and Sergei B. Vakulenko

Subjects

β-lactamase, OXA-23, Acinetobacter, inhibitor, carbapenem, crystal structure, Microbiology, QR1-502

Abstract

ABSTRACT Acinetobacter baumannii has become a major nosocomial pathogen, as it is often multidrug-resistant, which results in infections characterized by high mortality rates. The bacterium achieves high levels of resistance to β-lactam antibiotics by producing β-lactamases, enzymes which destroy these valuable agents. Historically, the carbapenem family of β-lactam antibiotics have been the drugs of choice for treating A. baumannii infections. However, their effectiveness has been significantly diminished due to the pathogen’s production of carbapenem-hydrolyzing class D β-lactamases (CHDLs); thus, new antibiotics and inhibitors of these enzymes are urgently needed. Here, we describe a new carbapenem antibiotic, MA-1-206, in which the canonical C6 hydroxyethyl group has been replaced with hydroxymethyl. The antimicrobial susceptibility studies presented here demonstrated that this compound is more potent than meropenem and imipenem against A. baumannii producing OXA-23, the most prevalent CHDL of this pathogen, and also against strains producing the CHDL OXA-24/40 and the class B metallo-β-lactamase VIM-2. Our kinetic and mass spectrometry studies revealed that this drug is a reversible inhibitor of OXA-23, where inhibition takes place through a branched pathway. X-ray crystallographic studies, molecular docking, and molecular dynamics simulations of the OXA-23-MA-1-206 complex show that the C6 hydroxymethyl group forms a hydrogen bond with the carboxylated catalytic lysine of OXA-23, effectively preventing deacylation. These results provide a promising strategy for designing a new generation of CHDL-resistant carbapenems to restore their efficacy against deadly A. baumannii infections. IMPORTANCE Carbapenem antibiotics are the drugs of choice for treatment of deadly infections caused by Gram-negative bacteria. However, their efficacy is severely compromised by the wide spread of carbapenem-hydrolyzing class D β-lactamases (CHDLs). The importance of this research is the discovery that substitution of the canonical hydroxyethyl group of carbapenems by a hydroxymethyl significantly enhances stability against inactivation by the major CHDL of Acinetobacter baumannii, OXA-23. These results provide a novel strategy for designing next-generation, carbapenemase-stable carbapenems to fight multidrug-resistant infections caused by Gram-negative pathogens.

Published

2022

4. Peptidoglycan reshaping by a noncanonical peptidase for helical cell shape in Campylobacter jejuni

Author

Kyungjin Min, Doo Ri An, Hye-Jin Yoon, Neha Rana, Ji Su Park, Jinshil Kim, Mijoon Lee, Dusan Hesek, Sangryeol Ryu, B. Moon Kim, Shahriar Mobashery, Se Won Suh, and Hyung Ho Lee

Subjects

Science

Abstract

Peptidoglycans (PG) define bacterial cell shapes. Here, the authors provide mechanistic insights into the peptidoglycan peptidase 3 (Pgp3) from the spiral shaped human pathogen Campylobacter jejuni by determining its crystal structure alone and in complex with synthetic cell-wall PG derivatives, and they further show that the enzyme has both d,d-endopeptidase and d,d-carboxypeptidase activities

Published

2020

5. Penetration through Outer Membrane and Efflux Potential in Pseudomonas aeruginosa of Bulgecin A as an Adjuvant to β-Lactam Antibiotics

Author

Choon Kim, Shusuke Tomoshige, Mijoon Lee, Helen I. Zgurskaya, and Shahriar Mobashery

Subjects

Pseudomonas aeruginosa, bulgecin A, β-lactam antibiotics, efflux pumps, porins, potentiation, Therapeutics. Pharmacology, RM1-950

Abstract

The treatment of infections by Gram-negative bacteria remains a difficult clinical challenge. In the light of the dearth of discovery of novel antibiotics, one strategy that is being explored is the use of adjuvants to enhance antibacterial activities of existing antibiotics. One such adjuvant is bulgecin A, which allows for the lowering of minimal-inhibitory concentrations for β-lactam antibiotics. We have shown that bulgecin A inhibits three of the pseudomonal lytic transglycosylases in its mode of action, yet high concentrations are needed for potentiation activity. Herein, we document that bulgecin A is not a substrate for pseudomonal efflux pumps, whose functions could have been a culprit in the need for high concentrations. We present evidence that the penetration barrier into the periplasm is at the root of the need for high concentrations of bulgecin A in its potentiation of β-lactam antibiotics.

Published

2023

6. Horizontal-Acquisition of a Promiscuous Peptidoglycan-Recycling Enzyme Enables Aphids To Influence Symbiont Cell Wall Metabolism

Author

Thomas E. Smith, Mijoon Lee, Maria D. Person, Dusan Hesek, Shahriar Mobashery, and Nancy A. Moran

Subjects

Buchnera, carboxypeptidase, cell wall, endopeptidase, enzyme promiscuity, horizontal gene transfer, Microbiology, QR1-502

Abstract

ABSTRACT During evolution, enzymes can undergo shifts in preferred substrates or in catalytic activities. An intriguing question is how enzyme function changes following horizontal gene transfer, especially for bacterial genes that have moved to animal genomes. Some insects have acquired genes that encode enzymes for the biosynthesis of bacterial cell wall components and that appear to function to support or control their obligate endosymbiotic bacteria. In aphids, the bacterial endosymbiont Buchnera aphidicola provides essential amino acids for aphid hosts but lacks most genes for remodeling of the bacterial cell wall. The aphid genome has acquired seven genes with putative functions in cell wall metabolism that are primarily expressed in the aphid cells harboring Buchnera. In analyses of aphid homogenates, we detected peptidoglycan (PGN) muropeptides indicative of the reactions of PGN hydrolases encoded by horizontally acquired aphid genes but not by Buchnera genes. We produced one such host enzyme, ApLdcA, and characterized its activity with both cell wall derived and synthetic PGN. Both ApLdcA and the homologous enzyme in Escherichia coli, which functions as an l,d-carboxypeptidase in the cytoplasmic PGN recycling pathway, exhibit turnover of PGN substrates containing stem pentapeptides and cross-linkages via l,d-endopeptidase activity, consistent with a potential role in cell wall remodeling. Our results suggest that ApLdcA derives its functions from the promiscuous activities of an ancestral LdcA enzyme, whose acquisition by the aphid genome may have enabled hosts to influence Buchnera cell wall metabolism as a means to control symbiont growth and division. IMPORTANCE Most enzymes are capable of performing biologically irrelevant side reactions. During evolution, promiscuous enzyme activities may acquire new biological roles, especially after horizontal gene transfer to new organisms. Pea aphids harbor obligate bacterial symbionts called Buchnera and encode horizontally acquired bacterial genes with putative roles in cell wall metabolism. Though Buchnera lacks cell wall endopeptidase genes, we found evidence of endopeptidase activity among peptidoglycan muropeptides purified from aphids. We characterized a multifunctional, aphid-encoded enzyme, ApLdcA, which displays l,d-endopeptidase activities considered promiscuous for the Escherichia coli homolog, for which these activities do not contribute to its native role in peptidoglycan recycling. These results exemplify the roles of enzyme promiscuity and horizontal gene transfer in enzyme evolution and demonstrate how aphids influence symbiont cell wall metabolism.

Published

2021

7. Structural basis of denuded glycan recognition by SPOR domains in bacterial cell division

Author

Martín Alcorlo, David A. Dik, Stefania De Benedetti, Kiran V. Mahasenan, Mijoon Lee, Teresa Domínguez-Gil, Dusan Hesek, Elena Lastochkin, Daniel López, Bill Boggess, Shahriar Mobashery, and Juan A. Hermoso

Subjects

Science

Abstract

SPOR domains are present in bacterial proteins that recognize cell-wall peptidoglycan strands stripped of the peptide stems. Here, Alcorlo et al. show that, indeed, the presence of peptide stems abrogates binding to a SPOR domain, and provide insights into the molecular basis for recognition.

Published

2019

8. Prophylactic Activation of Shh Signaling Attenuates TBI-Induced Seizures in Zebrafish by Modulating Glutamate Excitotoxicity through Eaat2a

Author

James Hentig, Leah J. Campbell, Kaylee Cloghessy, Mijoon Lee, William Boggess, and David R. Hyde

Subjects

traumatic brain injury, blunt-force TBI, post-traumatic seizures, zebrafish, sonic hedgehog signaling, purmorphamine, Biology (General), QH301-705.5

Abstract

Approximately 2 million individuals experience a traumatic brain injury (TBI) every year in the United States. Secondary injury begins within minutes after TBI, with alterations in cellular function and chemical signaling that contribute to excitotoxicity. Post-traumatic seizures (PTS) are experienced in an increasing number of TBI individuals that also display resistance to traditional anti-seizure medications (ASMs). Sonic hedgehog (Shh) is a signaling pathway that is upregulated following central nervous system damage in zebrafish and aids injury-induced regeneration. Using a modified Marmarou weight drop on adult zebrafish, we examined PTS following TBI and Shh modulation. We found that inhibiting Shh signaling by cyclopamine significantly increased PTS in TBI fish, prolonged the timeframe PTS was observed, and decreased survival across all TBI severities. Shh-inhibited TBI fish failed to respond to traditional ASMs, but were attenuated when treated with CNQX, which blocks ionotropic glutamate receptors. We found that the Smoothened agonist, purmorphamine, increased Eaat2a expression in undamaged brains compared to untreated controls, and purmorphamine treatment reduced glutamate excitotoxicity following TBI. Similarly, purmorphamine reduced PTS, edema, and cognitive deficits in TBI fish, while these pathologies were increased and/or prolonged in cyclopamine-treated TBI fish. However, the increased severity of TBI phenotypes with cyclopamine was reduced by cotreating fish with ceftriaxone, which induces Eaat2a expression. Collectively, these data suggest that Shh signaling induces Eaat2a expression and plays a role in regulating TBI-induced glutamate excitotoxicity and TBI sequelae.

Published

2021

9. Structural Basis of the Heterodimer Formation between Cell Shape-Determining Proteins Csd1 and Csd2 from Helicobacter pylori.

Author

Doo Ri An, Ha Na Im, Jun Young Jang, Hyoun Sook Kim, Jieun Kim, Hye Jin Yoon, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Soon-Jong Kim, and Se Won Suh

Subjects

Medicine, Science

Abstract

Colonization of the human gastric mucosa by Helicobacter pylori requires its high motility, which depends on the helical cell shape. In H. pylori, several genes (csd1, csd2, csd3/hdpA, ccmA, csd4, csd5, and csd6) play key roles in determining the cell shape by alteration of cross-linking or by trimming of peptidoglycan stem peptides. H. pylori Csd1, Csd2, and Csd3/HdpA are M23B metallopeptidase family members and may act as d,d-endopeptidases to cleave the d-Ala4-mDAP3 peptide bond of cross-linked dimer muropeptides. Csd3 functions also as the d,d-carboxypeptidase to cleave the d-Ala4-d-Ala5 bond of the muramyl pentapeptide. To provide a basis for understanding molecular functions of Csd1 and Csd2, we have carried out their structural characterizations. We have discovered that (i) Csd2 exists in monomer-dimer equilibrium and (ii) Csd1 and Csd2 form a heterodimer. We have determined crystal structures of the Csd2121-308 homodimer and the heterodimer between Csd1125-312 and Csd2121-308. Overall structures of Csd1125-312 and Csd2121-308 monomers are similar to each other, consisting of a helical domain and a LytM domain. The helical domains of both Csd1 and Csd2 play a key role in the formation of homodimers or heterodimers. The Csd1 LytM domain contains a catalytic site with a Zn2+ ion, which is coordinated by three conserved ligands and two water molecules, whereas the Csd2 LytM domain has incomplete metal ligands and no metal ion is bound. Structural knowledge of these proteins sheds light on the events that regulate the cell wall in H. pylori.

Published

2016

10. The external PASTA domain of the essential serine/threonine protein kinase PknB regulates mycobacterial growth

Author

Obolbek Turapov, Jessica Loraine, Christopher H. Jenkins, Philippe Barthe, Daniel McFeely, Francesca Forti, Daniela Ghisotti, Dusan Hesek, Mijoon Lee, Andrew R. Bottrill, Waldemar Vollmer, Shahriar Mobashery, Martin Cohen-Gonsaud, and Galina V. Mukamolova

Subjects

mycobacterium tuberculosis, serine/threonine protein kinase, magnesium, muropeptides, pknb, pasta domain, Biology (General), QH301-705.5

Abstract

PknB is an essential serine/threonine protein kinase required for mycobacterial cell division and cell-wall biosynthesis. Here we demonstrate that overexpression of the external PknB_PASTA domain in mycobacteria results in delayed regrowth, accumulation of elongated bacteria and increased sensitivity to β-lactam antibiotics. These changes are accompanied by altered production of certain enzymes involved in cell-wall biosynthesis as revealed by proteomics studies. The growth inhibition caused by overexpression of the PknB_PASTA domain is completely abolished by enhanced concentration of magnesium ions, but not muropeptides. Finally, we show that the addition of recombinant PASTA domain could prevent regrowth of Mycobacterium tuberculosis, and therefore offers an alternative opportunity to control replication of this pathogen. These results suggest that the PknB_PASTA domain is involved in regulation of peptidoglycan biosynthesis and maintenance of cell-wall architecture.

Published

2015

11. Structural and Functional Insights into Peptidoglycan Access for the Lytic Amidase LytA of Streptococcus pneumoniae

Author

Peter Mellroth, Tatyana Sandalova, Alexey Kikhney, Francisco Vilaplana, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Staffan Normark, Dmitri Svergun, Birgitta Henriques-Normark, and Adnane Achour

Subjects

Microbiology, QR1-502

Abstract

ABSTRACT The cytosolic N-acetylmuramoyl-l-alanine amidase LytA protein of Streptococcus pneumoniae, which is released by bacterial lysis, associates with the cell wall via its choline-binding motif. During exponential growth, LytA accesses its peptidoglycan substrate to cause lysis only when nascent peptidoglycan synthesis is stalled by nutrient starvation or β-lactam antibiotics. Here we present three-dimensional structures of LytA and establish the requirements for substrate binding and catalytic activity. The solution structure of the full-length LytA dimer reveals a peculiar fold, with the choline-binding domains forming a rigid V-shaped scaffold and the relatively more flexible amidase domains attached in a trans position. The 1.05-Å crystal structure of the amidase domain reveals a prominent Y-shaped binding crevice composed of three contiguous subregions, with a zinc-containing active site localized at the bottom of the branch point. Site-directed mutagenesis was employed to identify catalytic residues and to investigate the relative impact of potential substrate-interacting residues lining the binding crevice for the lytic activity of LytA. In vitro activity assays using defined muropeptide substrates reveal that LytA utilizes a large substrate recognition interface and requires large muropeptide substrates with several connected saccharides that interact with all subregions of the binding crevice for catalysis. We hypothesize that the substrate requirements restrict LytA to the sites on the cell wall where nascent peptidoglycan synthesis occurs. IMPORTANCE Streptococcus pneumoniae is a human respiratory tract pathogen responsible for millions of deaths annually. Its major pneumococcal autolysin, LytA, is required for autolysis and fratricidal lysis and functions as a virulence factor that facilitates the spread of toxins and factors involved in immune evasion. LytA is also activated by penicillin and vancomycin and is responsible for the lysis induced by these antibiotics. The factors that regulate the lytic activity of LytA are unclear, but it was recently demonstrated that control is at the level of substrate recognition and that LytA required access to the nascent peptidoglycan. The present study was undertaken to structurally and functionally investigate LytA and its substrate-interacting interface and to determine the requirements for substrate recognition and catalysis. Our results reveal that the amidase domain comprises a complex substrate-binding crevice and needs to interact with a large-motif epitope of peptidoglycan for catalysis.

Published

2014

12. The l,d-Transpeptidase Ldt

Author

Marta, Toth, Nichole K, Stewart, Clyde A, Smith, Mijoon, Lee, and Sergei B, Vakulenko

Subjects

Acinetobacter baumannii, Carbapenems, Peptidyl Transferases, Peptidoglycan, Anti-Bacterial Agents

Abstract

l,d-Transpeptidases (LDTs) are enzymes that catalyze reactions essential for biogenesis of the bacterial cell wall, including formation of 3-3 cross-linked peptidoglycan. Unlike the historically well-known bacterial transpeptidases, the penicillin-binding proteins (PBPs), LDTs are resistant to inhibition by the majority of β-lactam antibiotics, with the exception of carbapenems and penems, allowing bacteria to survive in the presence of these drugs. Here we report characterization of Ldt

Published

2023

13. The <scp>l,d</scp>-Transpeptidase LdtAb from Acinetobacter baumannii Is Poorly Inhibited by Carbapenems and Has a Unique Structural Architecture

Author

Marta Toth, Nichole K. Stewart, Clyde A. Smith, Mijoon Lee, and Sergei B. Vakulenko

Subjects

Infectious Diseases

Published

2022

14. Synthesis of Muramyl‐δ‐Lactam in Spore Peptidoglycan of Clostridioides difficile

Author

Choon Kim, Mijoon Lee, Biruk T. Birhanu, Dusan Hesek, Mayland Chang, and Shahriar Mobashery

Subjects

Organic Chemistry, Molecular Medicine, Molecular Biology, Biochemistry

Published

2023

15. Sleep Deficit as a Risk Factor for Hypertension in Korean Adults

Author

MIJOON LEE, Inmyung Song, and Bum Jeun Seo

Subjects

hypertension, health behavior, Renewable Energy, Sustainability and the Environment, adult, Geography, Planning and Development, sleep duration, Building and Construction, Management, Monitoring, Policy and Law

Abstract

This study aims to evaluate the association between sleep duration and hypertension in Korean adults aged 30 and older. This is a population-based cross-sectional study using the 2020 Korean National Health and Nutritional Examination Survey data. Study subjects numbered 3984 after excluding people with missing data for key exposures and outcome variables. Of the study subjects, 18.8% (n = 748) sleep for less than 6 h a day. Increased risk for hypertension was associated with being male, of old age, unemployed, of low educational achievement, and overweight, as well as drinking, smoking, stress, and short sleep duration. The prevalence of sleep deficit was associated with sex, age, education level, income, and health insurance type. Logistic regression analyses were performed to identify whether sleep duration affects the risk of hypertension. In the unadjusted model, the odds ratio (OR) of having hypertension was lower among people sleeping for 7.0–7.9 h (OR = 0.52, 95% confidence interval (95% CI) = 0.42–0.64) than those sleeping for fewer than 6 h per day. After adjusting for sociodemographic factors (sex, age, education level, occupation, and health insurance), the OR for 7.0–7.9 h remained significant (OR = 0.74, 95% CI = 0.59–0.92). This association was not significant when the model was further adjusted for health-related factors (smoking, drinking, physical activity, BMI level, and stress). Measures to promote adequate sleep duration should be included in programs to prevent and manage hypertension.

Published

2023

16. Turnover Chemistry and Structural Characterization of the Cj0843c Lytic Transglycosylase of Campylobacter jejuni

Author

Mijoon Lee, Shahriar Mobashery, Dusan Hesek, Focco van den Akker, Jacob Boorman, Elena Lastochkin, Ximin Zeng, Jun Lin, Snigdha A. Mathure, and Vijay Kumar

Subjects

chemistry.chemical_classification, 0303 health sciences, Mutation, biology, 030302 biochemistry & molecular biology, Mutagenesis, Active site, Peptide, medicine.disease_cause, biology.organism_classification, Biochemistry, Campylobacter jejuni, 03 medical and health sciences, chemistry.chemical_compound, Enzyme, Lytic cycle, chemistry, medicine, biology.protein, Peptidoglycan

Abstract

The soluble lytic transglycosylase Cj0843c from Campylobacter jejuni breaks down cell-wall peptidoglycan (PG). Its nonhydrolytic activity sustains cell-wall remodeling and repair. We report herein our structure-function studies probing the substrate preferences and recognition by this enzyme. Our studies show that Cj0843c exhibits both exolytic and endolytic activities and forms the N-acetyl-1,6-anhydromuramyl (anhMurNAc) peptidoglycan termini, the typical transformation catalyzed by lytic transglycosylase. Cj0843c shows a trend toward a preference for substrates with anhMurNAc ends and those with peptide stems. Mutagenesis revealed that the catalytic E390 is critical for activity. In addition, mutagenesis showed that R388 and K505, located in the positively charged pocket near E390, also serve important roles. Mutation of R326, on the opposite side of this positively charged pocket, enhanced activity. Our data point to different roles for positively charged residues in this pocket for productive binding of the predominantly negatively charged PG. We also show by X-ray crystallography and by molecular dynamics simulations that the active site of Cj0843c is still capable of binding GlcNAc containing di- and trisaccharides without MurNAc moieties, without peptide stems, and without the anhMurNAc ends.

Published

2021

17. Inhibition of the Clostridioides difficile Class D β-Lactamase CDD-1 by Avibactam

Author

Marta Toth, Mijoon Lee, Clyde A. Smith, Anastasiya Stasyuk, Sergei B. Vakulenko, and Nichole K. Stewart

Subjects

0301 basic medicine, chemistry.chemical_classification, biology, Avibactam, 030106 microbiology, biology.organism_classification, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Infectious Diseases, Enzyme, chemistry, Biochemistry, Pathogen, Bacteria, Clostridioides

Abstract

Avibactam is a potent diazobicyclooctane inhibitor of class A and C β-lactamases. The inhibitor also exhibits variable activity against some class D enzymes from Gram-negative bacteria; however, its interaction with recently discovered class D β-lactamases from Gram-positive bacteria has not been studied. Here, we describe microbiological, kinetic, and mass spectrometry studies of the interaction of avibactam with CDD-1, a class D β-lactamase from the clinically important pathogen Clostridioides difficile, and show that avibactam is a potent irreversible mechanism-based inhibitor of the enzyme. X-ray crystallographic studies at three time-points demonstrate the rapid formation of a stable CDD-1-avibactam acyl-enzyme complex and highlight differences in the anchoring of the inhibitor by class D enzymes from Gram-positive and Gram-negative bacteria.

Published

2021

18. Effects of Inactivation of d,d-Transpeptidases of Acinetobacter baumannii on Bacterial Growth and Susceptibility to β-Lactam Antibiotics

Author

Nichole K. Stewart, Mijoon Lee, Sergei B. Vakulenko, and Marta Toth

Subjects

Acinetobacter baumannii, Lysis, medicine.drug_class, Antibiotics, Mutant, Microbial Sensitivity Tests, Biology, Bacterial growth, beta-Lactams, Bacterial cell structure, Microbiology, chemistry.chemical_compound, Bacterial Proteins, Mechanisms of Resistance, polycyclic compounds, medicine, Penicillin-Binding Proteins, Pharmacology (medical), Gene, Pharmacology, biochemical phenomena, metabolism, and nutrition, biology.organism_classification, Anti-Bacterial Agents, Infectious Diseases, chemistry, Peptidyl Transferases, Peptidoglycan

Abstract

Resistance to β-lactams, the most used antibiotics worldwide, constitutes the major problem for the treatment of bacterial infections. In the nosocomial pathogen Acinetobacter baumannii, β-lactamase-mediated resistance to the carbapenem family of β-lactam antibiotics has resulted in the selection and dissemination of multidrug-resistant isolates, which often cause infections characterized by high mortality rates. There is thus an urgent demand for new β-lactamase-resistant antibiotics that also inhibit their targets, penicillin-binding proteins (PBPs). As some PBPs are indispensable for the biosynthesis of the bacterial cell wall and survival, we evaluated their importance for the growth of A. baumannii by performing gene inactivation studies of d,d-transpeptidase domains of high-molecular-mass (HMM) PBPs individually and in combination with one another. We show that PBP3 is essential for A. baumannii survival, as deletion mutants of this d,d-transpeptidase were not viable. The inactivation of PBP1a resulted in partial cell lysis and retardation of bacterial growth, and these effects were further enhanced by the additional inactivation of PBP2 but not PBP1b. Susceptibility to β-lactam antibiotics increased 4- to 8-fold for the A. baumannii PBP1a/PBP1b/PBP2 triple mutant and 2- to 4-fold for all remaining mutants. Analysis of the peptidoglycan structure revealed a significant change in the muropeptide composition of the triple mutant and demonstrated that the lack of d,d-transpeptidase activity of PBP1a, PBP1b, and PBP2 is compensated for by an increase in the l,d-transpeptidase-mediated cross-linking activity of LdtJ. Overall, our data showed that in addition to essential PBP3, the simultaneous inhibition of PBP1a and PBP2 or PBPs in combination with LdtJ could represent potential strategies for the design of novel drugs against A. baumannii.

Published

2022

19. Chemical Glycobiology

Author

Xi Chen, Randall Halcomb, Peng George Wang, Xiaomei Yu, George O'Doherty, Lijun Huang>, Xiaowei Lu, Xuefei Huang, Mijoon Lee, Dusan Hesek, Shahriar Mobashery, Zbigniew J. Witczak, Hai Yu, Harshal A. Chokhawala, Shengshu Huang, Xi Chen, Lai-Xi Wang, Suvarn S. Kulkarni, Jacquelyn Gervay-Hague, Chengfe

Published

2008

20. Integrative structural biology of the penicillin-binding protein-1 from Staphylococcus aureus, an essential component of the divisome machinery

Author

Kiran V. Mahasenan, Rhona Feltzer, Dusan Hesek, Mijoon Lee, Renee Bouley, Siseth Martínez-Caballero, Choon Kim, Jed F. Fisher, Shahriar Mobashery, Rafael Molina, Juan A. Hermoso, Inés G. Muñoz, Mayland Chang, National Institutes of Health (US), Ministerio de Economía y Competitividad (España), Ministerio de Ciencia, Innovación y Universidades (España), and ALBA Synchrotron

Subjects

Staphylococcus aureus, Penicillin binding proteins, PASTA domains, Antibiotics inhibition, SAXS in-solution structure, Biophysics, Peptidoglycan binding, Biochemistry, chemistry.chemical_compound, Structural Biology, Glycosyltransferase, Genetics, Divisome, ComputingMethodologies_COMPUTERGRAPHICS, biology, Molecular dynamics simulations, PBP1, X-ray crystal structure, PASTA domain, Computer Science Applications, Structural biology, chemistry, biology.protein, Penicillin Antibiotic, Peptidoglycan, Linker, TP248.13-248.65, Biotechnology, Research Article

Abstract

Graphical abstract, Highlights • X-ray crystallography, SAXS and MD simulations elucidates the 3D structure for saPBP1. • 3D structure of saPBP1 reveals dynamical mobility for the pedestal and PASTA domains. • Structures with β-lactams and penta-Gly provide model for peptidoglycan binding. • Mass-spectrometry reveals peptidoglycan binding by PASTA and the non-active-site regions. • Computation provides a dynamic model for full-length PBP1 and its complex with FtsW., The penicillin-binding proteins are the enzyme catalysts of the critical transpeptidation crosslinking polymerization reaction of bacterial peptidoglycan synthesis and the molecular targets of the penicillin antibiotics. Here, we report a combined crystallographic, small-angle X-ray scattering (SAXS) in-solution structure, computational and biophysical analysis of PBP1 of Staphylococcus aureus (saPBP1), providing mechanistic clues about its function and regulation during cell division. The structure reveals the pedestal domain, the transpeptidase domain, and most of the linker connecting to the “penicillin-binding protein and serine/threonine kinase associated” (PASTA) domains, but not its two PASTA domains, despite their presence in the construct. To address this absence, the structure of the PASTA domains was determined at 1.5 Å resolution. Extensive molecular-dynamics simulations interpret the PASTA domains of saPBP1 as conformationally mobile and separated from the transpeptidase domain. This conclusion was confirmed by SAXS experiments on the full-length protein in solution. A series of crystallographic complexes with β-lactam antibiotics (as inhibitors) and penta-Gly (as a substrate mimetic) allowed the molecular characterization of both inhibition by antibiotics and binding for the donor and acceptor peptidoglycan strands. Mass-spectrometry experiments with synthetic peptidoglycan fragments revealed binding by PASTA domains in coordination with the remaining domains. The observed mobility of the PASTA domain in saPBP1 could play a crucial role for in vivo interaction with its glycosyltransferase partner in the membrane or with other components of the divisome machinery, as well as for coordination of transpeptidation and polymerization processes in the bacterial divisome.

Published

2021

21. Catalytic Cycle of Glycoside Hydrolase BglX from Pseudomonas aeruginosa and Its Implications for Biofilm Formation

Author

Julia Sanz-Aparicio, Mijoon Lee, Kiran V. Mahasenan, María T. Batuecas, Shahriar Mobashery, Choon Kim, Juan A. Hermoso, Jed F. Fisher, Neha Rana, Stefania De Benedetti, Dusan Hesek, University of Notre Dame, Ministerio de Ciencia, Innovación y Universidades (España), ALBA Synchrotron, and National Institutes of Health (US)

Subjects

0301 basic medicine, 010405 organic chemistry, Stereochemistry, Pseudomonas aeruginosa, Mutant, Oxocarbenium, Biofilm, General Medicine, Periplasmic space, medicine.disease_cause, 01 natural sciences, Biochemistry, 0104 chemical sciences, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, Catalytic cycle, medicine, Molecular Medicine, Glycoside hydrolase, Peptidoglycan

Abstract

8 pags., 5 figs., BglX is a heretofore uncharacterized periplasmic glycoside hydrolase (GH) of the human pathogen Pseudomonas aeruginosa. X-ray analysis identifies it as a protein homodimer. The two active sites of the homodimer comprise catalytic residues provided by each monomer. This arrangement is seen in, The work at the University of Notre Dame was supported by grants from the National Institutes of Health (GM61629 and GM131685), and that in Spain by a grant from MICIU Ministry (BFU2017-90030-P). The authors thank the staff from the ALBA (Barcelona, Spain) synchrotron facility for help in X-ray data collection and CRC of the University of Notre Dame for the computing resources. The authors acknowledge Grant P30 DK089507 from the National Institutes of Health for the BglX transposon mutant of P. aeruginosa.

Published

2019

22. Structural basis of denuded glycan recognition by SPOR domains in bacterial cell division

Author

Daniel Lopez, Martín Alcorlo, Elena Lastochkin, Teresa Domínguez-Gil, Kiran V. Mahasenan, David A. Dik, Bill Boggess, Mijoon Lee, Shahriar Mobashery, Dusan Hesek, Stefania De Benedetti, Juan A. Hermoso, Ministerio de Economía y Competitividad (España), National Institutes of Health (US), University of Notre Dame, ALBA Synchrotron, SCOAP, and Ministerio de Ciencia, Innovación y Universidades (España)

Subjects

0301 basic medicine, Glycan, Cell division, Science, Lipoproteins, Protein domain, Glycobiology, General Physics and Astronomy, Peptide, Peptidoglycan, Plasma protein binding, Molecular Dynamics Simulation, Crystallography, X-Ray, 010402 general chemistry, 01 natural sciences, Article, General Biochemistry, Genetics and Molecular Biology, Bacterial cell structure, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, Cell Wall, Escherichia coli, lcsh:Science, X-ray crystallography, chemistry.chemical_classification, Bacterial structural biology, Multidisciplinary, biology, Escherichia coli Proteins, Proteins, General Chemistry, 0104 chemical sciences, 030104 developmental biology, Carbohydrate Sequence, chemistry, Biochemistry, Pseudomonas aeruginosa, biology.protein, lcsh:Q, Bacillus subtilis, Protein Binding

Abstract

13 pags., 9 figs. -- Open Access funded by Creative Commons Atribution Licence 4.0, SPOR domains are widely present in bacterial proteins that recognize cell-wall peptidoglycan strands stripped of the peptide stems. This type of peptidoglycan is enriched in the septal ring as a product of catalysis by cell-wall amidases that participate in the separation of daughter cells during cell division. Here, we document binding of synthetic denuded glycan ligands to the SPOR domain of the lytic transglycosylase RlpA from Pseudomonas aeruginosa (SPOR-RlpA) by mass spectrometry and structural analyses, and demonstrate that indeed the presence of peptide stems in the peptidoglycan abrogates binding. The crystal structures of the SPOR domain, in the apo state and in complex with different synthetic glycan ligands, provide insights into the molecular basis for recognition and delineate a conserved pattern in other SPOR domains. The biological and structural observations presented here are followed up by molecular-dynamics simulations and by exploration of the effect on binding of distinct peptidoglycan modifications., The work in Spain was supported by grants from the Spanish Ministry of Science, Innovation and Universities (BFU2014-59389-P and BFU2017-90030-P to JAH) and in the USA by grants from the NIH (GM131685 and GM61629 to SM). D.A.D. is a Fellow of the Chemistry-Biochemistry-Biology Interface Program (NIH Training Grant T32GM075762) and a Fellow of the ECK Institute of Global Health at the University of Notre Dame. We thank Dr. We thank the staff from ALBA synchrotron facility (Barcelona, Spain) for help during crystallographic data collection. We thank the Center for Research Computing of the University of Notre Dame for the computing resources.

Published

2019

23. Why Is Blood Glucose Control Important to Self-Care of Pregnant Women with Gestational Diabetes Mellitus?

Author

Yeon Kim, MIJOON LEE, and Bum Jeun Seo

Subjects

pregnant women, gestational diabetes mellitus, self-care, hemoglobin A1c, education, Renewable Energy, Sustainability and the Environment, Geography, Planning and Development, Building and Construction, Management, Monitoring, Policy and Law

Abstract

This study aimed to investigate the change in self-care, self-efficacy, and health status of pregnant women with gestational diabetes mellitus (GDM), and to identify whether blood glucose control influences pregnancy outcomes. This study is experimental research using a one-group pretest-posttest design. The study subjects were 40 pregnant women diagnosed with GDM, and the data were collected in their 24th and 40th week of gestation and analyzed using SPSS 27.0. Paired samples t-test was used to compare the health status, self-care, and self-efficacy of subjects between antepartum and postpartum, and t-test and non-parametric test were used to evaluate the changes in self-care and self-efficacy according to the ability to control blood glucose. As a result of this study, maternal BMI, self-care, and self-efficacy after childbirth were significantly worse than before (p < 0.001). However, HbA1c did not deteriorate and remained at a similar level, which is possibly the effect of diabetes education (p = 0.902). Furthermore, it was found that HbA1c control has a significant effect on preventing a decrease in self-care. In conclusion, it is necessary to develop and apply various diabetes education programs to manage blood glucose levels in pregnant women with GDM as blood glucose control is effective for improving not only their health outcomes but also their cognitive status, such as self-care.

Published

2022

24. Turnover chemistry and structural characterization of the Cj0843c lytic transglycosylase of Campylobacter jejuni

Author

Vijay Kumar, Jacob Boorman, Ximin Zeng, Focco van den Akker, Dusan Hesek, Snigdha A. Mathure, Jun Lin, Mijoon Lee, and Shahriar Mobashery

Subjects

biology, Lytic cycle, Chemistry, Genetics, biology.organism_classification, Molecular Biology, Biochemistry, Campylobacter jejuni, Biotechnology, Microbiology

Published

2021

25. Turnover Chemistry and Structural Characterization of the Cj0843c Lytic Transglycosylase of

Author

Vijay, Kumar, Snigdha A, Mathure, Mijoon, Lee, Jacob, Boorman, Ximin, Zeng, Jun, Lin, Dusan, Hesek, Elena, Lastochkin, Shahriar, Mobashery, and Focco, van den Akker

Subjects

Campylobacter jejuni, Mutagenesis, Protein Conformation, Glycosyltransferases, Molecular Dynamics Simulation, Article

Abstract

The soluble lytic transglycosylase Cj0843c from Campylobacter jejuni breaks down cell-wall peptidoglycan (PG). Its non-hydrolytic activity sustains cell-wall remodeling and repair. We report herein our structure-function studies probing the substrate preferences and recognition by this enzyme. Our studies show that Cj0843c exhibits both exolytic and endolytic activities and forms the N-acetyl-1,6-anhydromuramyl (anhMurNAc) peptidoglycan termini, the typical transformation catalyzed by lytic transglycosylase. Cj0843c shows a trend toward a preference of substrates with anhMurNAc ends and those with peptide stems. Mutagenesis revealed that the catalytic E390 is critical for activity. In addition, mutagenesis showed that R388 and K505, located in the positively charged pocket near E390, also serve important roles. Mutation of R326, on the opposite side of this positively charged pocket, enhanced activity. Our data point to different roles for positively charged residues in this pocket for productive binding of the predominantly negatively charged PG. We also show by X-ray crystallography and by MD simulations that the active site of Cj0843c is still capable of binding GlcNAc containing di- and trisaccharides without MurNAc moieties, without peptide stems, and without the anhMurNAc ends.

Published

2021

26. Inhibition of the

Author

Nichole K, Stewart, Marta, Toth, Anastasiya, Stasyuk, Mijoon, Lee, Clyde A, Smith, and Sergei B, Vakulenko

Subjects

Clostridioides, Gram-Negative Bacteria, Gram-Positive Bacteria, beta-Lactamase Inhibitors, Azabicyclo Compounds, beta-Lactamases, Article, Anti-Bacterial Agents

Abstract

Avibactam is a potent diazobicyclooctane inhibitor of class A and C β-lactamases. The inhibitor also exhibits variable activity against some class D enzymes from Gram-negative bacteria; however, its interaction with recently discovered class D β-lactamases from Gram-positive bacteria has not been studied. Here, we describe microbiological, kinetic, and mass spectrometry studies of the interaction of avibactam with CDD-1, a class D β-lactamase from the clinically important pathogen Clostridioides difficile, and show that avibactam is a potent irreversible mechanism-based inhibitor of the enzyme. X-ray crystallographic studies at three time-points demonstrate the rapid formation of a stable CDD-1-avibactam acyl–enzyme complex and highlight differences in the anchoring of the inhibitor by class D enzymes from Gram-positive and Gram-negative bacteria.

Published

2021

27. Selective MMP-9 Inhibitor (

Author

Zhihong, Peng, Trung T, Nguyen, Wei, Song, Bowen, Anderson, William R, Wolter, Valerie A, Schroeder, Dusan, Hesek, Mijoon, Lee, Shahriar, Mobashery, and Mayland, Chang

Abstract

[Image: see text] Diabetic foot ulcers (DFUs) are a common complication of diabetes that are recalcitrant to healing due to persistent inflammation. The majority of DFUs have bacterial biofilms, with Staphylococcus epidermidis as a predominant bacterium, requiring infection control with antibiotics before treatment of the wound. Matrix metalloproteinases (MMPs) play roles in the pathology and repair of DFUs. However, defining the roles of the 24 human MMPs has been challenging due to the presence of three forms for each MMP, of which only one is catalytically competent, and the lack of convenient methods to distinguish among the three forms of MMPs. Using an affinity resin that binds only to the active forms of MMPs, with identification and quantification by mass spectrometry, we found that infected wounds in mice had increased levels of active MMP-9 compared to uninfected ones, paralleling infected human DFUs. MMP-9 activity prevents diabetic wounds from healing. We evaluated the efficacy of the selective small-molecule MMP-9 inhibitor, (R)-ND-336, in the infected diabetic mouse model of wound healing and showed that (R)-ND-336 alone or in combination with the antibiotic linezolid improves wound healing by inhibiting the detrimental MMP-9, mitigating macrophage infiltration to diminish inflammation, and increasing angiogenesis to restore the normal wound healing process. An advantage of this strategy is the ability to administer (R)-ND-336 concurrently with an antibiotic.

Published

2020

28. The Streptococcal Protease SpeB Antagonizes the Biofilms of the Human PathogenStaphylococcus aureusUSA300 through Cleavage of the Staphylococcal SdrC Protein

Author

Victoria A. Ploplis, Francis J. Castellino, Mijoon Lee, Bill Boggess, Katelyn E. Carothers, Jeffrey A. Mayfield, Deborah L. Donahue, Shaun W. Lee, and Zhong Liang

Subjects

Staphylococcus aureus, Proteases, Streptococcus pyogenes, medicine.medical_treatment, Exotoxins, Virulence, Human pathogen, Biology, medicine.disease_cause, Microbiology, 03 medical and health sciences, Bacterial Proteins, Streptococcal Infections, medicine, Humans, Molecular Biology, 030304 developmental biology, 0303 health sciences, Protease, 030306 microbiology, Biofilm, Gene Expression Regulation, Bacterial, adhesins, Bacterial adhesin, Biofilms, proteases, SpeB, Research Article

Abstract

Streptococcus pyogenes (GAS) causes a range of diseases in humans, ranging from mild to severe, and produces many virulence factors in order to be a successful pathogen. One factor produced by many GAS strains is the protease SpeB, which has been studied for its ability to cleave and degrade human proteins, an important factor in GAS pathogenesis. An understudied aspect of SpeB is the manner in which its broad proteolytic activity affects other microorganisms that co-occupy niches similar to that of GAS. The significance of the research reported herein is the demonstration that SpeB can degrade the biofilms of the human pathogen Staphylococcus aureus, which has important implications for how SpeB may be utilized by GAS to successfully compete in a polymicrobial environment., Streptococcus pyogenes, or group A Streptococcus (GAS), is both a pathogen and an asymptomatic colonizer of human hosts and produces a large number of surface-expressed and secreted factors that contribute to a variety of infection outcomes. The GAS-secreted cysteine protease SpeB has been well studied for its effects on the human host; however, despite its broad proteolytic activity, studies on how this factor is utilized in polymicrobial environments are lacking. Here, we utilized various forms of SpeB protease to evaluate its antimicrobial and antibiofilm properties against the clinically important human colonizer Staphylococcus aureus, which occupies niches similar to those of GAS. For our investigation, we used a skin-tropic GAS strain, AP53CovS+, and its isogenic ΔspeB mutant to compare the production and activity of native SpeB protease. We also generated active and inactive forms of recombinant purified SpeB for functional studies. We demonstrate that SpeB exhibits potent biofilm disruption activity at multiple stages of S. aureus biofilm formation. We hypothesized that the surface-expressed adhesin SdrC in S. aureus was cleaved by SpeB, which contributed to the observed biofilm disruption. Indeed, we found that SpeB cleaved recombinant SdrC in vitro and in the context of the full S. aureus biofilm. Our results suggest an understudied role for the broadly proteolytic SpeB as an important factor for GAS colonization and competition with other microorganisms in its niche. IMPORTANCE Streptococcus pyogenes (GAS) causes a range of diseases in humans, ranging from mild to severe, and produces many virulence factors in order to be a successful pathogen. One factor produced by many GAS strains is the protease SpeB, which has been studied for its ability to cleave and degrade human proteins, an important factor in GAS pathogenesis. An understudied aspect of SpeB is the manner in which its broad proteolytic activity affects other microorganisms that co-occupy niches similar to that of GAS. The significance of the research reported herein is the demonstration that SpeB can degrade the biofilms of the human pathogen Staphylococcus aureus, which has important implications for how SpeB may be utilized by GAS to successfully compete in a polymicrobial environment.

Published

2020

29. Peptidoglycan reshaping by a noncanonical peptidase for helical cell shape in Campylobacter jejuni

Author

Mijoon Lee, Shahriar Mobashery, Kyungjin Min, Se Won Suh, Doo Ri An, B. Moon Kim, Dusan Hesek, Neha Rana, Jinshil Kim, Hye-Jin Yoon, Ji Su Park, Sangryeol Ryu, and Hyung Ho Lee

Subjects

Models, Molecular, 0301 basic medicine, Protein Conformation, Virulence Factors, Science, 030106 microbiology, General Physics and Astronomy, Peptidoglycan, Crystallography, X-Ray, Biochemistry, Campylobacter jejuni, Article, Citric Acid, General Biochemistry, Genetics and Molecular Biology, Bacterial cell structure, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, Bacterial Proteins, Catalytic Domain, Endopeptidases, Hydrolase, lcsh:Science, X-ray crystallography, Multidisciplinary, biology, Chemistry, Hydrolysis, Active site, General Chemistry, biology.organism_classification, Cell biology, 030104 developmental biology, Mutation, Metalloproteases, biology.protein, lcsh:Q, Pathogens, Peptidoglycan binding

Abstract

Assembly of the peptidoglycan is crucial in maintaining viability of bacteria and in defining bacterial cell shapes, both of which are important for existence in the ecological niche that the organism occupies. Here, eight crystal structures for a member of the cell-shape-determining class of Campylobacter jejuni, the peptidoglycan peptidase 3 (Pgp3), are reported. Characterization of the turnover chemistry of Pgp3 reveals cell wall d,d-endopeptidase and d,d-carboxypeptidase activities. Catalysis is accompanied by large conformational changes upon peptidoglycan binding, whereby a loop regulates access to the active site. Furthermore, prior hydrolysis of the crosslinked peptide stem from the saccharide backbone of the peptidoglycan on one side is a pre-requisite for its recognition and turnover by Pgp3. These analyses reveal the noncanonical nature of the transformations at the core of the events that define the morphological shape for C. jejuni as an intestinal pathogen., Peptidoglycans (PG) define bacterial cell shapes. Here, the authors provide mechanistic insights into the peptidoglycan peptidase 3 (Pgp3) from the spiral shaped human pathogen Campylobacter jejuni by determining its crystal structure alone and in complex with synthetic cell-wall PG derivatives, and they further show that the enzyme has both d,d-endopeptidase and d,d-carboxypeptidase activities

Published

2020

30. Key side products due to reactivity of dimethylmaleoyl moiety as amine protective group

Author

Dusan Hesek, Bruce C. Noll, Mijoon Lee, and Shahriar Mobashery

Subjects

General Chemical Engineering, Hydrazine, General Chemistry, Biochemistry, Industrial and Manufacturing Engineering, Article, chemistry.chemical_compound, chemistry, Nucleophile, Group (periodic table), Electrophile, Materials Chemistry, Organic chemistry, Moiety, Organic synthesis, Reactivity (chemistry), Amine gas treating

Abstract

Dimethylmaleoyl (DMM) moiety has become an important amine protective group in sugar chemistry. We disclose herein that DMM-containing D-glucosamine analogues, because of their electrophilic nature, are prone to reactions with strong nucleophiles, such as hydrazine, resulting in a set of undesired side products that are difficult to detect, yet proved to be problematic for organic synthesis.

Published

2020

31. Transforming growth factor β (TGF-β) receptor signaling regulates kinase networks and phosphatidylinositol metabolism during T-cell activation

Author

William C. Boggess, Mijoon Lee, William F. Hawse, and Richard T. Cattley

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, T-Lymphocytes, Immunology, SMAD, Lymphocyte Activation, Phosphatidylinositols, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Phosphatidylinositol 3-Kinases, Enzyme Stability, PTEN, Tensin, Animals, Phosphatidylinositol, Smad3 Protein, Phosphorylation, Phosphotyrosine, Molecular Biology, PI3K/AKT/mTOR pathway, Smad4 Protein, ZAP-70 Protein-Tyrosine Kinase, 030102 biochemistry & molecular biology, biology, Kinase, Chemistry, PTEN Phosphohydrolase, Cell Biology, Cell biology, Enzyme Activation, Mice, Inbred C57BL, 030104 developmental biology, Lymphocyte Specific Protein Tyrosine Kinase p56(lck), biology.protein, Protein Multimerization, Receptors, Transforming Growth Factor beta, Proto-oncogene tyrosine-protein kinase Src, Protein Binding, Signal Transduction

Abstract

The cytokine content in tissue microenvironments shapes the functional capacity of a T cell. This capacity depends on the integration of extracellular signaling through multiple receptors, including the T-cell receptor (TCR), co-receptors, and cytokine receptors. Transforming growth factor β (TGF-β) signals through its cognate receptor, TGFβR, to SMAD family member proteins and contributes to the generation of a transcriptional program that promotes regulatory T-cell differentiation. In addition to transcription, here we identified specific signaling networks that are regulated by TGFβR. Using an array of biochemical approaches, including immunoblotting, kinase assays, immunoprecipitation, and flow cytometry, we found that TGFβR signaling promotes the formation of a SMAD3/4-protein kinase A (PKA) complex that activates C-terminal Src kinase (CSK) and thereby down-regulates kinases involved in proximal TCR activation. Additionally, TGFβR signaling potentiated CSK phosphorylation of the P85 subunit in the P85–P110 phosphoinositide 3-kinase (PI3K) heterodimer, which reduced PI3K activity and down-regulated the activation of proteins that require phosphatidylinositol (3,4,5)-trisphosphate (PtdIns(3,4,5)P3) for their activation. Moreover, TGFβR-mediated disruption of the P85–P110 interaction enabled P85 binding to a lipid phosphatase, phosphatase and tensin homolog (PTEN), aiding in the maintenance of PTEN abundance and thereby promoting elevated PtdIns(4,5)P2 levels in response to TGFβR signaling. Taken together, these results highlight that TGF-β influences the trajectory of early T-cell activation by altering PI3K activity and PtdIns levels.

Published

2020

32. A Structural Dissection of the Active Site of the Lytic Transglycosylase MltE from Escherichia coli

Author

Mijoon Lee, Shahriar Mobashery, Elena Lastochkin, Kiran V. Mahasenan, Jed F. Fisher, María T. Batuecas, Juan A. Hermoso, David A. Dik, Daniel R. Marous, and Ministerio de Economía y Competitividad (España)

Subjects

0301 basic medicine, Mutation, Missense, 010402 general chemistry, Cleavage (embryo), medicine.disease_cause, 01 natural sciences, Biochemistry, Catalysis, Bacterial cell structure, 03 medical and health sciences, Catalytic Domain, medicine, Escherichia coli, chemistry.chemical_classification, Escherichia coli K12, biology, Chemistry, Escherichia coli Proteins, Wild type, Glycosyltransferases, Active site, Lyase, 0104 chemical sciences, 030104 developmental biology, Enzyme, Amino Acid Substitution, Lytic cycle, biology.protein

Abstract

Lytic transglycosylases (LTs) are bacterial enzymes that catalyze the cleavage of the glycan strands of the bacterial cell wall. The mechanism of this cleavage is a remarkable intramolecular transacetalization reaction, accomplished by an ensemble of active-site residues. Because the LT reaction occurs in parallel with the cell wall bond-forming reactions catalyzed by the penicillin-binding proteins, simultaneous inhibition of both enzymes can be particularly bactericidal to Gram-negative bacteria. The MltE lytic transglycosylase is the smallest of the eight LTs encoded by the Escherichia coli genome. Prior crystallographic and computational studies identified four active-site residues - E64, S73, S75, and Y192 - as playing roles in catalysis. Each of these four residues was individually altered by mutation to give four variant enzymes (E64Q, S73A, S75A, and Y192F). All four variants showed reduced catalytic activity [soluble wild type (100%) > soluble Y192F and S75A (both 40%) > S73A (4%) > E64Q (≤1%)]. The crystal structure of each variant protein was determined at the resolution of 2.12 Å for E64Q, 2.33 Å for Y192F, 1.38 Å for S73A, and 1.35 Å for S75A. These variants show alteration of the hydrogen-bond interactions of the active site. Within the framework of a prior computational study of the LT mechanism, we suggest the mechanistic role of these four active-site residues in MltE catalysis.

Published

2018

33. Expression of active matrix metalloproteinase-9 as a likely contributor to the clinical failure of aclerastide in treatment of diabetic foot ulcers

Author

Matthew M. Champion, Dusan Hesek, Trung T. Nguyen, Rocio L. Pérez, Valerie A. Schroeder, Mark A. Suckow, Mijoon Lee, Shahriar Mobashery, William R. Wolter, Derong Ding, and Mayland Chang

Subjects

0301 basic medicine, medicine.medical_specialty, 030209 endocrinology & metabolism, Matrix metalloproteinase, Gastroenterology, Article, Gene Expression Regulation, Enzymologic, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, medicine, Animals, Treatment Failure, Pharmacology, Wound Healing, Peptide analog, integumentary system, business.industry, Angiotensin II, medicine.disease, Diabetic foot, Diabetic Foot, Up-Regulation, Clinical trial, Matrix Metalloproteinase 8, 030104 developmental biology, Matrix Metalloproteinase 9, Female, Wound healing, business, Complication

Abstract

Chronic wounds are a complication of diabetes. Treatment for diabetic foot ulcers is complex with little clinical recourse, resulting in 108,000 lower-limb amputations annually in the United States alone. Matrix metalloproteinases (MMPs) play important roles in the pathology and in the repair of chronic wounds. We previously identified active MMP-8 and MMP-9 in wounds of diabetic mice and determined that MMP-8 accelerates wound repair, while MMP-9 is the culprit for the diabetic wound being refractory to healing. Aclerastide, a peptide analog of angiotensin II, recently failed in phase III clinical trials for treatment of diabetic foot ulcers. We demonstrate herein that treatment of wounds of diabetic mice with aclerastide results in elevated levels of reactive oxygen species and of active MMP-9, which is likely an important contributor to the failure of aclerastide in clinical trials.

Published

2018

34. Synergistic and additive interactions between receptor signaling networks drive the regulatory T cell versus T helper 17 cell fate choice

Author

Corey W. Shipman, William F. Hawse, Douglas S. Prado, William C. Boggess, Richard T. Cattley, Cassandra Happe, Matthew L. MacDonald, and Mijoon Lee

Subjects

TGF-βR, TGF-β receptor, Regulatory T cell, medicine.medical_treatment, Receptors, Antigen, T-Cell, T cell differentiation, chemical and pharmacologic phenomena, Cell fate determination, T-Lymphocytes, Regulatory, Biochemistry, Cell Line, TEAB, triethylammonium bicarbonate, proteomics, ITK, interlukin-2-inducible T-cell kinase, medicine, Animals, T helper 17 cell, T regulatory cell, Receptor, Molecular Biology, Cells, Cultured, PI3K/AKT/mTOR pathway, TCR, T cell receptor, Chemistry, T-cell receptor, hemic and immune systems, Cell Biology, Receptors, Interleukin-6, phospholipid signaling, Cell biology, Mice, Inbred C57BL, Treg, Treg, T regulatory cell, medicine.anatomical_structure, Cytokine, Th17 Cells, Th17, T helper 17 cell, Th17, JAK, Janus kinase, Receptors, Transforming Growth Factor beta, IL-6R, IL-6 receptor, Signal Transduction, Research Article

Abstract

CD4+ T cells differentiate into subsets that promote immunity or minimize damage to the host. T helper 17 cells (Th17) are effector cells that function in inflammatory responses. T regulatory cells (Tregs) maintain tolerance and prevent autoimmunity by secreting immunosuppressive cytokines and expressing check point receptors. While the functions of Th17 and Treg cells are different, both cell fate trajectories require T cell receptor (TCR) and TGF-β receptor (TGF-βR) signals, and Th17 polarization requires an additional IL-6 receptor (IL-6R) signal. Utilizing high-resolution phosphoproteomics, we identified that both synergistic and additive interactions between TCR, TGF-βR, and IL-6R shape kinase signaling networks to differentially regulate key pathways during the early phase of Treg versus Th17 induction. Quantitative biochemical analysis revealed that CD4+ T cells integrate receptor signals via SMAD3, which is a mediator of TGF-βR signaling. Treg induction potentiates the formation of the canonical SMAD3/4 trimer to activate a negative feedback loop through kinases PKA and CSK to suppress TCR signaling, phosphatidylinositol metabolism, and mTOR signaling. IL-6R signaling activates STAT3 to bind SMAD3 and block formation of the SMAD3/4 trimer during the early phase of Th17 induction, which leads to elevated TCR and PI3K signaling. These data provide a biochemical mechanism by which CD4+ T cells integrate TCR, TGF-β, and IL-6 signals via generation of alternate SMAD3 complexes that control the development of early signaling networks to potentiate the choice of Treg versus Th17 cell fate.

Published

2021

35. Deciphering the Nature of Enzymatic Modifications of Bacterial Cell Walls

Author

Mijoon Lee, Shahriar Mobashery, Elena Lastochkin, Dusan Hesek, David A. Dik, and Bill Boggess

Subjects

0301 basic medicine, Glycoside Hydrolases, Lysin, Peptidoglycan, Biology, 010402 general chemistry, 01 natural sciences, Biochemistry, Mass Spectrometry, Article, Bacterial cell structure, Substrate Specificity, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Cell Wall, Multienzyme Complexes, Transferases, Endopeptidases, Molecular Biology, Chromatography, High Pressure Liquid, Organism, chemistry.chemical_classification, Bacteria, Organic Chemistry, Streptomyces griseus, Substrate (biology), biology.organism_classification, Recombinant Proteins, Enzymes, 0104 chemical sciences, 030104 developmental biology, Enzyme, chemistry, Pseudomonas aeruginosa, Biocatalysis, Molecular Medicine

Abstract

The major constituent of bacterial cell wall is peptidoglycan, which in its crosslinked form is a polymer of considerable complexity that encases the entire bacterium. A functional cell wall is indispensable for the survival of the organism. There are several dozens of enzymes that assemble and disassemble the peptidoglycan dynamically within each bacterial generation. Understanding of the nature of these transformations is critical knowledge on these events. Octasaccharide peptidoglycans were prepared and studied with seven recombinant cell-wall-active enzymes (SltB1, MltB, RlpA, mutanolysin, AmpDh2, AmpDh3 and PBP5). With the use of highly sensitive mass spectrometry methods, we describe the breadth of reactions that these enzymes catalyze with the peptidoglycan and shed light on the nature of the cell-wall alteration performed by these enzymes. The enzymes exhibit broadly distinct preferences for their substrate peptidoglycans in the reactions that they catalyze.

Published

2017

36. From Genome to Proteome to Elucidation of Reactions for All Eleven Known Lytic Transglycosylases from Pseudomonas aeruginosa

Author

Elena Lastochkin, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Jed F. Fisher, David A. Dik, Jennifer Fishovitz, and Bill Boggess

Subjects

0301 basic medicine, Proteome, Molecular Conformation, 010402 general chemistry, medicine.disease_cause, 01 natural sciences, Article, Catalysis, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Cell Wall, medicine, Organic chemistry, Pathogen, chemistry.chemical_classification, biology, Chemistry, Pseudomonas aeruginosa, Glycosyltransferases, General Medicine, General Chemistry, biology.organism_classification, 0104 chemical sciences, 030104 developmental biology, Enzyme, Lytic cycle, Biochemistry, Biocatalysis, lipids (amino acids, peptides, and proteins), Peptidoglycan, Bacteria

Abstract

An enzyme superfamily, the lytic transglycosylases (LTs), occupies the space between the two membranes of Gram-negative bacteria. LTs catalyze the non-hydrolytic cleavage of the bacterial peptidoglycan cell-wall polymer. This reaction is central to the growth of the cell wall, for excavating the cell wall for protein insertion, and for monitoring the cell wall so as to initiate resistance responses to cell-wall-acting antibiotics. The nefarious Gram-negative pathogen Pseudomonas aeruginosa encodes eleven LTs. With few exceptions, their substrates and functions are unknown. Each P. aeruginosa LT was expressed as a soluble protein and evaluated with a panel of substrates (both simple and complex mimetics of their natural substrates). Thirty-one distinct products distinguish these LTs with respect to substrate recognition, catalytic activity, and relative exolytic or endolytic ability. These properties are foundational to an understanding of the LTs as catalysts and as antibiotic targets.

Published

2017

37. Synthesis and shift-reagent-assisted full NMR assignment of bacterial (Z8,E2,ω)-undecaprenol

Author

Mijoon Lee, Shahriar Mobashery, Jaroslav Zajicek, Dusan Hesek, and Jed F. Fisher

Subjects

010405 organic chemistry, Glycobiology, Stereochemistry, Metals and Alloys, General Chemistry, 010402 general chemistry, 01 natural sciences, Catalysis, 0104 chemical sciences, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, chemistry.chemical_compound, chemistry, Reagent, Materials Chemistry, Ceramics and Composites, Proton NMR, Isoprene, Carbanion

Abstract

The repeating isoprene unit is a fundamental biosynthetic motif. The repetitive structure presents challenges both for synthesis and for structural characterization. In this synthesis of the (Z8,E2,ω)-undecaprenol of prokaryotic glycobiology, we exemplify solutions to these challenges. Allylation of sulfone-derived carbanions controlled the stereochemistry, and its proof-of-structure was secured by Eu(hfc)3 complexation to disperse the overlaid resonances of its 1H NMR spectrum.

Published

2017

38. Hyperbaric oxygen therapy accelerates wound healing in diabetic mice by decreasing active matrix metalloproteinase-9

Author

William R. Wolter, Rocio L. Pérez, Dusan Hesek, Trung T. Nguyen, Mayland Chang, Valerie A. Schroeder, Mark A. Suckow, Mijoon Lee, Shahriar Mobashery, Matthew M. Champion, and Jeffrey I. Jones

Subjects

Dermatology, Matrix metalloproteinase, Pharmacology, Superoxide dismutase, 030207 dermatology & venereal diseases, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Animals, chemistry.chemical_classification, Reactive oxygen species, Enzyme Precursors, Glutathione Peroxidase, Hyperbaric Oxygenation, Wound Healing, biology, business.industry, Superoxide Dismutase, Hypoxia (medical), medicine.disease, Catalase, Diabetic foot, Diabetic Foot, Disease Models, Animal, Diabetic foot ulcer, chemistry, Diabetes Mellitus, Type 2, Matrix Metalloproteinase 9, biology.protein, Receptors, Leptin, Surgery, medicine.symptom, business, Wound healing, Reactive Oxygen Species

Abstract

Diabetic foot ulcers are characterized by hypoxia. For many patients, hyperbaric oxygen (HBO) therapy is the last recourse for saving the limb from amputation, for which the molecular basis is not understood. We previously identified the active form of matrix metalloproteinase-9 (MMP-9) as responsible for diabetic foot ulcer's recalcitrance to healing. Transcription of mmp-9 to the inactive zymogen is upregulated during hypoxia. Activation of the zymogen is promoted by proteases and reactive oxygen species (ROS). We hypothesized that the dynamics of these two events might lead to a lowering of active MMP-9 levels in the wounded tissue. We employed the full-thickness excisional db/db mouse model to study wound healing, and treated the mice to 3.0 atm of molecular oxygen for 90 minutes, 5 days per week for 10 days in an HBO research chamber. Treatment with HBO accelerated diabetic wound healing compared to untreated mice, with more completed and extended reepithelialization. We imaged the wounds for ROS in vivo with a luminol-based probe and found that HBO treatment actually decreases ROS levels. The levels of superoxide dismutase, catalase, and glutathione peroxidase-enzymes that turn over ROS-increased after HBO treatment, hence the observation of decreased ROS. Since ROS levels are lowered, we explored the effect that this would have on activation of MMP-9. Quantitative analysis with an affinity resin that binds and pulls down the active MMPs exclusively, coupled with proteomics, revealed that HBO treatment indeed reduces the active MMP-9 levels. This work for the first time demonstrates that diminution of active MMP-9 is a contributing factor and a mechanism for enhancement of diabetic wound healing by HBO therapy.

Published

2019

39. The Type VI Secretion System of Pseudomonas aeruginosa Delivers a Cell-Wall Amidase to Target Bacterial Competitors

Author

Min Wu, Haihua Liang, Yue Shi, Tietao Wang, Xiao Du, Mijoon Lee, Shahriar Mobashery, Zhaoyu Hu, and Dusan Hesek

Subjects

Proteases, biology, Pseudomonas aeruginosa, Periplasmic space, medicine.disease_cause, biology.organism_classification, Cell wall, chemistry.chemical_compound, chemistry, Biochemistry, medicine, Peptidoglycan, Bacterial outer membrane, Bacteria, Type VI secretion system

Abstract

The human pathogen Pseudomonas aeruginosa harbors three paralogous zinc proteases annotated as AmpD, AmpDh2, and AmpDh3, which turn over the cell wall and cell-wall-derived muropeptides. AmpD is cytoplasmic and plays a role in recycling of cell-wall muropeptides, with a link to antibiotic resistance. AmpDh2 and AmpDh3 are periplasmic enzymes; with the former anchored to the inner leaflet of the outer membrane and the latter a soluble enzyme. We document herein that the type VI secretion system locus II (H2-T6SS) of P. aeruginosa delivers AmpDh3 (but not AmpD or AmpDh2) to the periplasm of a prey bacterium upon contact. AmpDh3 hydrolyzes the cell-wall peptidoglycan of the prey bacterium, which leads to its killing, thereby providing a growth advantage for P. aerugionsa in bacterial competition. We also document that the periplasmic protein PA0808, heretofore of unknown function, affords self-protection from lysis by AmpDh3. Cognates of the AmpDh3-PA0808 pair are widely distributed across Gram-negative bacteria, underscoring the importance of their function as an evolutionary advantage and that of the H2-T6SS as the means for manifestation of the effect.

Published

2019

40. Lytic transglycosylases LtgA and LtgD perform distinct roles in remodeling, recycling and releasing peptidoglycan inNeisseria gonorrhoeae

Author

Ryan E. Schaub, Joseph P. Dillard, Yolande A. Chan, Dusan Hesek, Mijoon Lee, and Shahriar Mobashery

Subjects

0301 basic medicine, chemistry.chemical_classification, Biology, medicine.disease_cause, Microbiology, Proinflammatory cytokine, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Enzyme, Lytic cycle, Biochemistry, chemistry, Cytoplasm, Pelvic inflammatory disease, Neisseria gonorrhoeae, medicine, Tetrasaccharide, Peptidoglycan, Molecular Biology

Abstract

Neisseria gonorrhoeae releases peptidoglycan (PG) fragments during infection that provoke a large inflammatory response and, in pelvic inflammatory disease, this response leads to the death and sloughing of ciliated cells of the Fallopian tube. We characterized the biochemical functions and localization of two enzymes responsible for the release of proinflammatory PG fragments. The putative lytic transglycosylases LtgA and LtgD were shown to create the 1,6-anhydromuramyl moieties, and both enzymes were able to digest a small, synthetic tetrasaccharide dipeptide PG fragment into the cognate 1,6-anhydromuramyl-containing reaction products. Degradation of tetrasaccharide PG fragments by LtgA is the first demonstration of a family 1 lytic transglycosylase exhibiting this activity. Pulse-chase experiments in gonococci demonstrated that LtgA produces a larger amount of PG fragments than LtgD, and a vast majority of these fragments are recycled. In contrast, LtgD was necessary for wild-type levels of PG precursor incorporation and produced fragments predominantly released from the cell. Additionally, super-resolution microscopy established that LtgA localizes to the septum, whereas LtgD is localized around the cell. This investigation suggests a model where LtgD produces PG monomers in such a way that these fragments are released, whereas LtgA creates fragments that are mostly taken into the cytoplasm for recycling.

Published

2016

41. The crystal structure of the major pneumococcal autolysin LytA in complex with a large peptidoglycan fragment reveals the pivotal role of glycans for lytic activity

Author

Birgitta Henriques-Normark, Dusan Hesek, Tatyana Sandalova, Mijoon Lee, Shahriar Mobashery, Adnane Achour, and Peter Mellroth

Subjects

0301 basic medicine, Glycan, biology, 030106 microbiology, Autolysin, Ligand (biochemistry), Microbiology, Amidase, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, chemistry, Biochemistry, Hydrolase, biology.protein, Peptidoglycan, N-acetylmuramoyl-L-alanine amidase, Molecular Biology, DNA

Abstract

Summary The pneumococcal autolysin LytA is a key virulence factor involved in several important functions including DNA competence, immune evasion and biofilm formation. Here, we present the 1.05 A crystal structure of the catalytic domain of LytA in complex with a synthetic cell-wall-based peptidoglycan (PG) ligand that occupies the entire Y-shaped substrate-binding crevice. As many as twenty-one amino-acid residues are engaged in ligand interactions with a majority of these interactions directed towards the glycan strand. All saccharides are intimately bound through hydrogen bond, van der Waals and CH-π interactions. Importantly, the structure of LytA is not altered upon ligand binding, whereas the bound ligand assumes a different conformation compared to the unbound NMR-based solution structure of the same PG-fragment. Mutational study reveals that several non-catalytic glycan-interacting residues, structurally conserved in other amidases from Gram-positive Firmicutes, are pivotal for enzymatic activity. The three-dimensional structure of the LytA/PG complex provides a novel structural basis for ligand restriction by the pneumococcal autolysin, revealing for the first time an importance of the multivalent binding to PG saccharides.

Published

2016

42. Muropeptides in Pseudomonas aeruginosa and their Role as Elicitors of β‐Lactam‐Antibiotic Resistance

Author

Bill Boggess, Supurna Dhar, Stefania De Benedetti, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Kalai Mathee, and Blas Blázquez

Subjects

0301 basic medicine, Cell signaling, medicine.drug_class, 030106 microbiology, Antibiotics, Molecular Conformation, 010402 general chemistry, beta-Lactams, medicine.disease_cause, 01 natural sciences, Pentapeptide repeat, beta-Lactam Resistance, beta-Lactamases, Catalysis, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, medicine, biology, Pseudomonas aeruginosa, General Medicine, General Chemistry, biology.organism_classification, 0104 chemical sciences, Anti-Bacterial Agents, Metabolic pathway, Biochemistry, chemistry, Peptidoglycan, Peptides, Bacteria

Abstract

Muropeptides are a group of bacterial natural products generated from the cell wall in the course of its turnover. These compounds are cell-wall recycling intermediates and are also involved in signaling within the bacterium. However, the identity of these signaling molecules remains elusive. The identification and characterization of 20 muropeptides from Pseudomonas aeruginosa is described. The least abundant of these metabolites is present at 100 and the most abundant at 55,000 molecules per bacterium. Analysis of these muropeptides under conditions of induction of resistance to a β-lactam antibiotic identified two signaling muropeptides (N-acetylglucosamine-1,6-anhydro-N-acetylmuramyl pentapeptide and 1,6-anhydro-N-acetylmuramyl pentapeptide). Authentic synthetic samples of these metabolites were shown to activate expression of β-lactamase in the absence of any β-lactam antibiotic, thus indicating that they serve as chemical signals in this complex biochemical pathway.

Published

2016

43. Validation of Matrix Metalloproteinase-9 (MMP-9) as a Novel Target for Treatment of Diabetic Foot Ulcers in Humans and Discovery of a Potent and Selective Small-Molecule MMP-9 Inhibitor That Accelerates Healing

Author

Matthew M. Champion, Mark A. Suckow, Mijoon Lee, Shahriar Mobashery, William R. Wolter, Rocio L. Pérez, Mayland Chang, Valerie A. Schroeder, Elena Lastochkin, Charles E. Peterson, Dusan Hesek, Margaret K. Rose, Jeffrey I. Jones, Kiran V. Mahasenan, Derong Ding, and Trung T. Nguyen

Subjects

0301 basic medicine, Proteomics, Pharmacology, Matrix metalloproteinase, Matrix Metalloproteinase Inhibitors, Sulfides, Diabetes Mellitus, Experimental, 03 medical and health sciences, Methylamines, Mice, 0302 clinical medicine, Downregulation and upregulation, Becaplermin, Diabetes mellitus, Drug Discovery, medicine, Animals, Humans, Metalloproteinase, Wound Healing, Chemistry, Drug discovery, medicine.disease, Diabetic foot, Diabetic Foot, Mice, Inbred C57BL, 030104 developmental biology, Matrix Metalloproteinase 9, 030220 oncology & carcinogenesis, Molecular Medicine, Female, Wound healing, medicine.drug

Abstract

Diabetic foot ulcers (DFUs) are a significant health problem. A single existing FDA-approved drug for this ailment, becaplermin, is not standard-of-care. We previously demonstrated that upregulation of active matrix metalloproteinase (MMP)-9 is the reason that the diabetic wound in mice is recalcitrant to healing and that MMP-8 participates in wound repair. In the present study, we validate the target MMP-9 by identifying and quantifying active MMP-8 and MMP-9 in human diabetic wounds using an affinity resin that binds exclusively to the active forms of MMPs coupled with proteomics. Furthermore, we synthesize and evaluate enantiomerically pure ( R)- and ( S)-ND-336, as inhibitors of the detrimental MMP-9, and show that the ( R)-enantiomer has superior efficacy in wound healing over becaplermin. Our results reveal that the mechanisms of pathology and repair are similar in diabetic mice and diabetic humans and that ( R)-ND-336 holds promise for the treatment of DFUs as a first-in-class therapeutic.

Published

2018

44. Exolytic and endolytic turnover of peptidoglycan by lytic transglycosylase Slt of Pseudomonas aeruginosa

Author

Kiran V. Mahasenan, Isabel Usón, Mijoon Lee, Shahriar Mobashery, Juan A. Hermoso, Dusan Hesek, David A. Dik, Shusuke Tomoshige, Claudia Millán, Teresa Domínguez-Gil, María T. Batuecas, Elena Lastochkin, Agencia Estatal de Investigación (España), National Institutes of Health (US), Ministerio de Economía y Competitividad (España), University of Notre Dame, and Ministerio de Economía, Industria y Competitividad (España)

Subjects

0301 basic medicine, Glycan, Peptidog, genetic structures, 010402 general chemistry, 01 natural sciences, Bacterial cell structure, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Lycanlytic transglycosylases, chemistry.chemical_classification, Cell-wall recycling, Multidisciplinary, biology, Active site, Glycosidic bond, Lyase, 0104 chemical sciences, 030104 developmental biology, Enzyme, Biochemistry, chemistry, biology.protein, Peptidoglycan

Abstract

β-Lactam antibiotics inhibit cell-wall transpeptidases, preventing the peptidoglycan, the major constituent of the bacterial cell wall, from cross-linking. This causes accumulation of long non–cross-linked strands of peptidoglycan, which leads to bacterial death. Pseudomonas aeruginosa, a nefarious bacterial pathogen, attempts to repair this aberrantly formed peptidoglycan by the function of the lytic transglycosylase Slt. We document in this report that Slt turns over the peptidoglycan by both exolytic and endolytic reactions, which cause glycosidic bond scission from a terminus or in the middle of the peptidoglycan, respectively. These reactions were characterized with complex synthetic peptidoglycan fragments that ranged in size from tetrasaccharides to octasaccharides. The X-ray structure of the wild-type apo Slt revealed it to be a doughnut-shaped protein. In a series of six additional X-ray crystal structures, we provide insights with authentic substrates into how Slt is enabled for catalysis for both the endolytic and exolytic reactions. The substrate for the exolytic reaction binds Slt in a canonical arrangement and reveals how both the glycan chain and the peptide stems are recognized by the Slt. We document that the apo enzyme does not have a fully formed active site for the endolytic reaction. However, binding of the peptidoglycan at the existing subsites within the catalytic domain causes a conformational change in the protein that assembles the surface for binding of a more expansive peptidoglycan between the catalytic domain and an adjacent domain. The complexes of Slt with synthetic peptidoglycan substrates provide an unprecedented snapshot of the endolytic reaction., The work in the United States was supported by NIH Grant GM61629 (to S.M.), and in Madrid, Spain, by Spanish Ministry of Economy and Competitiveness Grants BFU2014-59389-P and BFU2017-90030-P (to J.A.H.). D.A.D. is a Fellow of the Chemistry–Biochemistry–Biology Interface Program (NIH Training Grant T32GM075762) and a Fellow of the Eck Institute of Global Health at the University of Notre Dame. Grants BIO2015-64216-P (to C.M.), MDM2014- 0435-01 (to I.U.), and BES-2015-071397 scholarship (to C.M.) supported the work in Barcelona, Spain.

Published

2018

45. Exolytic and endolytic turnover of peptidoglycan by lytic transglycosylase Slt of

Author

Mijoon, Lee, María T, Batuecas, Shusuke, Tomoshige, Teresa, Domínguez-Gil, Kiran V, Mahasenan, David A, Dik, Dusan, Hesek, Claudia, Millán, Isabel, Usón, Elena, Lastochkin, Juan A, Hermoso, and Shahriar, Mobashery

Subjects

Structure-Activity Relationship, Bacterial Proteins, Glycoside Hydrolases, Protein Domains, Pseudomonas aeruginosa, Peptidoglycan, Biological Sciences, Crystallography, X-Ray

Abstract

β-Lactam antibiotics are currently the most broadly used class of antibiotics. These antibiotics prevent bacterial cell wall from cross-linking, which leads to the accumulation of long non–cross-linked strands of peptidoglycan. Pseudomonas aeruginosa, a nefarious bacterial pathogen, attempts to repair this aberrantly formed peptidoglycan by the function of the lytic transglycosylase Slt. We document in the present report that Slt turns over the peptidoglycan by both scission of the glycosidic bonds from a terminus or in the middle of the peptidoglycan. In a series of seven X-ray crystal structures, we provide structural context to how these two reactions take place. These results disclose the details of bacterial response to the β-lactam antibiotic challenge.

Published

2018

46. Allostery, Recognition of Nascent Peptidoglycan, and Cross-linking of the Cell Wall by the Essential Penicillin-Binding Protein 2x of Streptococcus pneumoniae

Author

María T. Batuecas, Noelia Bernardo-García, Juan A. Hermoso, Kiran V. Mahasenan, Pavel Branny, Denisa Petráčková, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Linda Doubravová, and Ministerio de Economía y Competitividad (España)

Subjects

0301 basic medicine, Penicillin binding proteins, Peptidoglycan, Molecular Dynamics Simulation, 010402 general chemistry, Crystallography, X-Ray, 01 natural sciences, Biochemistry, Bacterial cell structure, Cell wall, 03 medical and health sciences, chemistry.chemical_compound, Molecular recognition, Cell Wall, Catalytic Domain, polycyclic compounds, Penicillin-Binding Proteins, Cephalosporin Antibiotic, biology, Active site, General Medicine, 0104 chemical sciences, 030104 developmental biology, Streptococcus pneumoniae, chemistry, biology.protein, Biocatalysis, Molecular Medicine, Penicillin Antibiotic

Abstract

Transpeptidases, members of the penicillin-binding protein (PBP) families, catalyze cross-linking of the bacterial cell wall. This transformation is critical for the survival of bacteria, and it is the target of inhibition by β-lactam antibiotics. We report herein our structural insights into catalysis by the essential PBP2x of Streptococcus pneumoniae by disclosing a total of four X-ray structures, two computational models based on the crystal structures, and molecular-dynamics simulations. The X-ray structures are for the apo PBP2x, the enzyme modified covalently in the active site by oxacillin (a penicillin antibiotic), the enzyme modified by oxacillin in the presence of a synthetic tetrasaccharide surrogate for the cell-wall peptidoglycan, and a noncovalent complex of cefepime (a cephalosporin antibiotic) bound to the active site. A prerequisite for catalysis by transpeptidases, including PBP2x, is the molecular recognition of nascent peptidoglycan strands, which harbor pentapeptide stems. We disclose that the recognition of nascent peptidoglycan by PBP2x takes place by complexation of one pentapeptide stem at an allosteric site located in the PASTA domains of this enzyme. This binding predisposes the third pentapeptide stem in the same nascent peptidoglycan strand to penetration into the active site for the turnover events. The complexation of the two pentapeptide stems in the same peptidoglycan strand is a recognition motif for the nascent peptidoglycan, critical for the cell-wall cross-linking reaction.

Published

2018

47. The Cell Shape-determining Csd6 Protein from Helicobacter pylori Constitutes a New Family of l,d-Carboxypeptidase

Author

Nam Ki Lee, Jakyung Yoo, Se Won Suh, Soon-Jong Kim, Byung Woo Han, Ha Na Im, Minghua Cui, Cheol-Hee Kim, Hyejin Yoon, Jun Young Jang, Byung Il Lee, Sun Choi, Jin Young Kim, Geul Bang, Dusan Hesek, Mijoon Lee, Shahriar Mobashery, Hyoun Sook Kim, Doo Ri An, and Ji Young Yoon

Subjects

Models, Molecular, Molecular Sequence Data, Carboxypeptidases, cell motility, peptidoglycan, Flagellum, flagellin, Biochemistry, structure-function, cell shape, Sugar acids, HP0518, L,D-carboxypeptidase, chemistry.chemical_compound, Protein structure, Catalytic Domain, Humans, Csd6, Amino Acid Sequence, protein structure, Molecular Biology, Peptide sequence, chemistry.chemical_classification, Helicobacter pylori, biology, Sugar Acids, Cell Biology, Carboxypeptidase, chemistry, Protein Structure and Folding, biology.protein, Peptidoglycan, Protein Multimerization, Function (biology), Flagellin

Abstract

Background: Csd6 is one of the cell shape-determining proteins in H. pylori. Results: The active site of Csd6 is tailored to function as an l,d-carboxypeptidase in the peptidoglycan-trimming process. Conclusion: Csd6 constitutes a new family of l,d-carboxypeptidase. Significance: The substrate limitation of Csd6 is a strategy that H. pylori uses to regulate its helical cell shape and motility., Helicobacter pylori causes gastrointestinal diseases, including gastric cancer. Its high motility in the viscous gastric mucosa facilitates colonization of the human stomach and depends on the helical cell shape and the flagella. In H. pylori, Csd6 is one of the cell shape-determining proteins that play key roles in alteration of cross-linking or by trimming of peptidoglycan muropeptides. Csd6 is also involved in deglycosylation of the flagellar protein FlaA. To better understand its function, biochemical, biophysical, and structural characterizations were carried out. We show that Csd6 has a three-domain architecture and exists as a dimer in solution. The N-terminal domain plays a key role in dimerization. The middle catalytic domain resembles those of l,d-transpeptidases, but its pocket-shaped active site is uniquely defined by the four loops I to IV, among which loops I and III show the most distinct variations from the known l,d-transpeptidases. Mass analyses confirm that Csd6 functions only as an l,d-carboxypeptidase and not as an l,d-transpeptidase. The d-Ala-complexed structure suggests possible binding modes of both the substrate and product to the catalytic domain. The C-terminal nuclear transport factor 2-like domain possesses a deep pocket for possible binding of pseudaminic acid, and in silico docking supports its role in deglycosylation of flagellin. On the basis of these findings, it is proposed that H. pylori Csd6 and its homologs constitute a new family of l,d-carboxypeptidase. This work provides insights into the function of Csd6 in regulating the helical cell shape and motility of H. pylori.

Published

2015

48. Water-Soluble MMP-9 Inhibitor Reduces Lesion Volume after Severe Traumatic Brain Injury

Author

Mayland Chang, Jiancun Cui, María Raquel Juárez, Dusan Hesek, Elena Lastochkin, Zezong Gu, Valerie A. Schroeder, Brittany N. Tomlinson, Rasheeq Nizam, Zhenzhou Chen, William R. Wolter, Mark A. Suckow, Major Gooyit, Mijoon Lee, Shahriar Mobashery, and Bill Boggess

Subjects

Male, Physiology, Traumatic brain injury, Cognitive Neuroscience, Lesion volume, Matrix Metalloproteinase Inhibitors, Matrix metalloproteinase, Pharmacology, Biochemistry, Article, Cell Line, Heterocyclic Compounds, 1-Ring, Inhibitory Concentration 50, Mice, Animal model, Pharmacokinetics, medicine, Animals, Distribution (pharmacology), Sulfones, Neurologic Examination, Dose-Response Relationship, Drug, business.industry, Water, Cell Biology, General Medicine, Prodrug, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Water soluble, Matrix Metalloproteinase 9, Solubility, Blood-Brain Barrier, Area Under Curve, Brain Injuries, business, Psychomotor Performance

Abstract

SB-3CT is a potent and selective inhibitor of matrix metalloproteinase (MMP)-2 and -9, which has shown efficacy in an animal model of severe traumatic brain injury (TBI). However, SB-3CT is poorly water-soluble and is metabolized primarily to p-hydroxy SB-3CT (2), a more potent inhibitor than SB-3CT. We synthesized the O-phosphate prodrug (3) of compound 2 to enhance its water solubility by more than 2000-fold. The prodrug 3 was a poor MMP inhibitor, but readily hydrolyzed to the active 2 in human blood. Pharmacokinetics and brain distribution studies in mice showed that 2 crossed the blood-brain barrier (BBB) and achieved therapeutic concentrations in the brain. The prodrug 3/compound 2 was evaluated in a mouse model of severe TBI and found to significantly decrease the brain lesion volume and improve neurological outcomes. MMP-9 inhibition by a water-soluble thiirane inhibitor is a promising therapy for treatment of TBI.

Published

2015

49. Regioselective Control of the SNAr Amination of 5-Substituted-2,4-Dichloropyrimidines Using Tertiary Amine Nucleophiles

Author

Dušan Hesek, Allen G. Oliver, Jed F. Fisher, Mijoon Lee, Shahriar Mobashery, and Tomas Rucil

Subjects

Molecular Structure, Tertiary amine, Organic Chemistry, Substituent, Regioselectivity, Stereoisomerism, Medicinal chemistry, Catalysis, chemistry.chemical_compound, Pyrimidines, chemistry, Nucleophile, Nucleophilic aromatic substitution, Organic chemistry, Amine gas treating, Amines, Selectivity, Amination

Abstract

The SNAr reaction of 2,4-dichloropyrimidines, further substituted with an electron-withdrawing substituent at C-5, has selectivity for substitution at C-4. Here we report that tertiary amine nucleophiles show excellent C-2 selectivity. In situ N-dealkylation of an intermediate gives the product that formally corresponds to the reaction of a secondary amine nucleophile at C-2. This reaction is practical (fast under simple reaction conditions, with good generality for tertiary amine structure and moderate to excellent yields) and significantly expands access to pyrimidine structures.

Published

2015

50. Synthesis and Evaluation of 1,2,4-Triazolo[1,5-a]pyrimidines as Antibacterial Agents Against Enterococcus faecium

Author

Huan Wang, Mijoon Lee, Shahriar Mobashery, Zhihong Peng, Elena Lastochkin, Blas Blázquez, Malika Kumarasiri, Renee Bouley, and Mayland Chang

Subjects

Penicillin binding proteins, Enterococcus faecium, Drug Evaluation, Preclinical, Chemistry Techniques, Synthetic, Microbial Sensitivity Tests, Article, Microbiology, Structure-Activity Relationship, Antibiotic resistance, Bacterial Proteins, Drug Stability, Cell Wall, Intensive care, Drug Discovery, Humans, Penicillin-Binding Proteins, Structure–activity relationship, biology, Chemistry, Triazoles, biology.organism_classification, Antimicrobial, Anti-Bacterial Agents, Pyrimidines, Biochemistry, Molecular Medicine, Antibacterial activity, Bacteria

Abstract

Rapid emergence of antibiotic resistance is one of the most challenging global public health concerns. In particular, vancomycin-resistant Enterococcus faecium infections have been increasing in frequency, representing 25% of enterococci infections in intensive care units. A novel class of 1,2,4-triazolo[1,5-a]pyrimidines active against E. faecium is reported herein. We used a three-component Biginelli-like heterocyclization reaction for the synthesis of a series of these derivatives based on reactions of aldehydes, β-dicarbonyl compounds, and 3-alkylthio-5-amino-1,2,4-triazoles. The resulting compounds were assayed for antimicrobial activity against the ESKAPE panel of bacteria, followed by investigation of their in vitro activities. These analyses identified a subset of 1,2,4-triazolo[1,5-a]pyrimidines that had good narrow-spectrum antibacterial activity against E. faecium and exhibited metabolic stability with low intrinsic clearance. Macromolecular synthesis assays revealed cell-wall biosynthesis as the target of these antibiotics.

Published

2015